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免疫抑制对于成功进行后肾的同种异体移植至关重要。

Immunosuppression is essential for successful allogeneic transplantation of the metanephros.

作者信息

Clancy Marc J, Marshall Damian, Dilworth Mark, Bottomley Martyn, Ashton Nick, Brenchley Paul

机构信息

Transplant unit, Western Infirmary, Glasgow G11 6NT, Scotland.

出版信息

Transplantation. 2009 Jul 27;88(2):151-9. doi: 10.1097/TP.0b013e3181abbe9d.

DOI:10.1097/TP.0b013e3181abbe9d
PMID:19623009
Abstract

BACKGROUND

Transplanted metanephroi vascularize and develop features of mature kidney. One group reported the intriguing finding that metanephric allografts and congenic, major histocompatibility complex-mismatched grafts developed without rejection in the absence of immunosuppression. Our experiments aim to investigate the hypothesis that metanephroi lack immunogenicity and identify immunosuppressives that do not inhibit development.

METHODS

We transplanted syngeneic metanephric grafts, allografts, and class II mismatched transplants to adult rats along with control grafts to nude recipients. glomerular filtration rates (GFRs) were measured where possible and transplants assessed by histology, immunohistochemistry, electron microscopy, and polymerase chain reaction.

RESULTS

Allografts underwent reliable growth and vascularization followed by vigorous rejection (n>200). Rejection was conserved across a class II-mismatched strain and when the earliest dissectable metanephric structures were transplanted. Immunosuppressive drugs other than cyclosporine demonstrated no in vivo toxicity to transplants and treatment with FTY720 and tacrolimus could ablate histologic evidence of allograft rejection. Syngeneic transplants exhibited function of up to 8% of a normal GFR. Renal mass reduction and growth factor treatment was associated with higher GFR than controls. The anatomical site of implantation was also linked strongly with achieved function.

CONCLUSIONS

Fetal kidney rudiments can provide a source of functioning renal tissue. These results suggest that such structures are no less immunogenic than mature organs, but the observed rejection is controllable.

摘要

背景

移植的后肾能够血管化并发育出成熟肾脏的特征。一组研究人员报告了一个有趣的发现,即后肾同种异体移植物以及同基因、主要组织相容性复合体不匹配的移植物在没有免疫抑制的情况下能够发育且不发生排斥反应。我们的实验旨在研究后肾缺乏免疫原性这一假说,并确定不抑制发育的免疫抑制剂。

方法

我们将同基因后肾移植物、同种异体移植物和II类不匹配移植物移植到成年大鼠体内,同时将对照移植物移植到裸鼠体内。尽可能测量肾小球滤过率(GFR),并通过组织学、免疫组织化学、电子显微镜和聚合酶链反应对移植物进行评估。

结果

同种异体移植物经历了可靠的生长和血管化,随后发生强烈排斥反应(n>200)。在II类不匹配的品系中以及移植最早可解剖的后肾结构时,排斥反应均会发生。除环孢素外的免疫抑制药物在体内对移植物均无毒性,用FTY720和他克莫司治疗可消除同种异体移植物排斥反应的组织学证据。同基因移植物表现出的功能可达正常GFR的8%。肾脏质量减轻和生长因子治疗与比对照组更高的GFR相关。植入的解剖部位也与所实现的功能密切相关。

结论

胎儿肾原基可提供功能性肾组织来源。这些结果表明,此类结构的免疫原性并不低于成熟器官,但观察到的排斥反应是可控的。

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